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甲状腺相关眼病中的肌肉自身抗原:分子遗传学的局限性

Muscle autoantigens in thyroid associated ophthalmopathy: the limits of molecular genetics.

作者信息

Elisei R, Weightman D, Kendall-Taylor P, Vassart G, Ludgate M

机构信息

IRIBHN, ULB, Bruxelles, Belgium.

出版信息

J Endocrinol Invest. 1993 Jul-Aug;16(7):533-40. doi: 10.1007/BF03348900.

Abstract

Unlike autoimmune thyroid disease (AITD) in which a number of autoantigens have been identified and characterized, the situation in thyroid associated ophthalmopathy (TAO) is far from clear. A number of candidate antigens have been identified by probing Western blots of orbital tissue (OT) with sera from TAO patients, the most frequently cited being proteins of molecular weight 23, 28, 55, 64, 78 and 120 kilodaltons. In an attempt to identify autoantigens in TAO we have produced a lambda gt11 human eye muscle expression library. This has been screened with sera from four patients with severe TAO whose antibodies bind to one or more of the aforementioned candidate antigens or to a thyroglobulin/acetylcholinesterase (Tg/Ache) shared epitope. Four clones were isolated and characterized; clone R14 encodes the carboxyl terminal 193 amino acids of an IgE binding protein, clones R10 and R13 encode unknown proteins having significant similarity with heat shock protein 27 and the U1 small nuclear ribonucleoprotein respectively. Clone R1 encodes an unknown peptide of 347 amino acids having no similarity with proteins in available data banks. R1 clone affinity purified autoantibodies bind to a protein of Mr 78 kD in a Western blot of porcine eye muscle tissue. Autoantibodies to the R1 recombinant lysogen were clearly demonstrated in 5 of 20 sera from Graves disease patients, its role merits further investigation. The possible relevance of these clones to the pathogenesis of TAO is discussed as well as the limitations of this type of approach in the identification of unknown autoantigens.

摘要

与自身免疫性甲状腺疾病(AITD)不同,在AITD中已鉴定并表征了多种自身抗原,而甲状腺相关眼病(TAO)的情况却远未明确。通过用TAO患者的血清探测眼眶组织(OT)的蛋白质免疫印迹,已鉴定出多种候选抗原,最常被提及的是分子量为23、28、55、64、78和120千道尔顿的蛋白质。为了鉴定TAO中的自身抗原,我们构建了一个λgt11人眼肌表达文库。用来自四名严重TAO患者的血清对其进行筛选,这些患者的抗体与上述一种或多种候选抗原或与甲状腺球蛋白/乙酰胆碱酯酶(Tg/Ache)共享表位结合。分离并鉴定了四个克隆;克隆R14编码一种IgE结合蛋白的羧基末端193个氨基酸,克隆R10和R13分别编码与热休克蛋白27和U1小核核糖核蛋白具有显著相似性的未知蛋白。克隆R1编码一个由347个氨基酸组成的未知肽段,与现有数据库中的蛋白质没有相似性。R1克隆亲和纯化的自身抗体在猪眼肌组织的蛋白质免疫印迹中与一种分子量为78 kD的蛋白质结合。在20例Graves病患者的血清中,有5例清楚地显示出针对R1重组溶原菌的自身抗体,其作用值得进一步研究。讨论了这些克隆与TAO发病机制的可能相关性以及这种方法在鉴定未知自身抗原方面的局限性。

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